Findings of Research Misconduct, 8091-8093 [2018-03766]
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Federal Register / Vol. 83, No. 37 / Friday, February 23, 2018 / Notices
Human Research Protections (SACHRP)
will hold a meeting that will be open to
the public. Information about SACHRP
and the full meeting agenda will be
posted on the SACHRP website at:
https://www.dhhs.gov/ohrp/sachrpcommittee/meetings/.
DATES: The meeting will be held on
Tuesday, March 13, 2018, from 8:30
a.m. until 5:00 p.m., and Wednesday,
March 14, 2018, from 8:30 a.m. until
4:00 p.m.
ADDRESSES: Fishers Lane Conference
Center, Terrace Level, 5635 Fishers
Lane, Rockville, Maryland 20852.
FOR FURTHER INFORMATION CONTACT: Julia
Gorey, J.D., Executive Director,
SACHRP; U.S. Department of Health
and Human Services, 1101 Wootton
Parkway, Suite 200, Rockville,
Maryland 20852; telephone: 240–453–
8141; fax: 240–453–6909; email address:
SACHRP@hhs.gov.
SUPPLEMENTARY INFORMATION: Under the
authority of 42 U.S.C. 217a, Section 222
of the Public Health Service Act, as
amended, SACHRP was established to
provide expert advice and
recommendations to the Secretary of
Health and Human Services (HHS),
through the Assistant Secretary for
Health, on issues and topics pertaining
to or associated with the protection of
human research subjects.
The Subpart A Subcommittee (SAS)
was established by SACHRP in October
2006 and is charged with developing
recommendations for consideration by
SACHRP regarding the application of
subpart A of 45 CFR part 46 in the
current research environment.
The Subcommittee on Harmonization
(SOH) was established by SACHRP at its
July 2009 meeting and charged with
identifying and prioritizing areas in
which regulations and/or guidelines for
human subjects research adopted by
various agencies or offices within HHS
would benefit from harmonization,
consistency, clarity, simplification and/
or coordination.
The SACHRP meeting will open to the
public at 8:30 a.m., on Tuesday, March
13, 2018, followed by opening remarks
from Dr. Jerry Menikoff, Director of the
Office for Human Research Protections
and Dr. Stephen Rosenfeld, SACHRP
Chair.
The SAS and SOH subcommittees
will present their recommendations
regarding the description of ‘‘key
information,’’ as required by the revised
Common Rule’s § 46.116(a)(5)(i). This
will be followed by a discussion of SOH
recommendations on the research use of
repositories and registries under various
consent models, under both the current
and the revised Common Rule. The
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Tuesday, March 13, meeting will
adjourn at approximately 5:00 p.m.
The Wednesday, March 14, meeting
will begin at 8:30 a.m. The SOH will
present and discuss recommendations
on the European Union’s General Data
Protection Regulation and its impact on
U.S. human subjects research.
Modifications to the previous day’s
work will be discussed and finalized.
The meeting will adjourn at
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Note that public comment must be
relevant to issues currently being
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comment should email or fax their
comments to SACHRP at SACHRP@
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to the meeting.
Public attendance at the meeting is
limited to space available. Individuals
who plan to attend and need special
assistance, such as sign language
interpretation or other reasonable
accommodations, should notify the
designated SACHRP point of contact at
the address/phone number listed above
at least one week prior to the meeting.
Dated: February 16, 2018.
Julia G. Gorey,
Executive Director, Secretary’s Advisory
Committee on Human Research Protections.
[FR Doc. 2018–03768 Filed 2–22–18; 8:45 am]
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DEPARTMENT OF HEALTH AND
HUMAN SERVICES
Office of the Secretary
Findings of Research Misconduct
Office of the Secretary, HHS.
Notice.
AGENCY:
ACTION:
Findings of research
misconduct have been made on the part
of Colleen T. Skau, Ph.D., former
postdoctoral fellow in the Cell Biology
and Physiology Center, National Heart,
Lung, and Blood Institute (NHLBI),
National Institutes of Health (NIH). Dr.
Skau engaged in research misconduct in
research supported by NHLBI, NIH. The
administrative actions, including three
(3) years of supervision, were
implemented beginning on January 25,
2018, and are detailed below.
FOR FURTHER INFORMATION CONTACT:
Wanda K. Jones, Ph.D., Interim Director,
Office of Research Integrity, 1101
Wootton Parkway, Suite 750, Rockville,
MD 20852, (240) 453–8200.
SUMMARY:
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SUPPLEMENTARY INFORMATION:
Colleen T. Skau, Ph.D., National
Institutes of Health: Based on
Respondent’s admission, an assessment
conducted by NIH, and analysis
conducted by ORI in its oversight
review, ORI found that Dr. Colleen T.
Skau, former postdoctoral fellow in the
Cell Biology and Physiology Center,
NHLBI, NIH, engaged in research
misconduct in research supported by
NHLBI, NIH.
ORI found that Respondent engaged
in research misconduct by intentionally,
knowingly, or recklessly reporting
falsified and/or fabricated data and/or
falsifying and/or fabricating data in the
following two (2) papers:
• Cell 167(6):1571–1585, 2016
(hereafter referred to as ‘‘Paper 1’’)
• Proceedings of the National Academy
of Sciences 112(19):E2447–E2456,
2015 (hereafter referred to as ‘‘Paper
2’’)
ORI found that Respondent engaged
in research misconduct by intentional,
knowing, or reckless falsification and/or
fabrication of the research record by
selectively reporting by inappropriate
inclusion/omission or alteration of data
points in ten (10) figures and falsely
reporting the statistical significance
based on falsified data in ten (10) figures
across the two (2) papers and
supplementary material. Specifically,
ORI found that:
• In Paper 1, Respondent falsified
and/or fabricated the research record in:
—Figure 3B, by selectively omitting/
including data points in the Rescue
condition
—Figure 5B, by reporting a significant
difference between conditions by
performing statistical calculations
based on fabricated primary data
—Figure 5C (bottom), by selectively
omitting images and conditions from
the analysis
—Figure 6I (bottom left), by reporting
data from the same data set as Figure
6B (top)
—Figure S5B, by reporting statistical
significance despite performing a T
test calculation that returned an
insignificant p-value
—Figure 7F, by reporting that error bars
represented standard deviation, when
they actually represented standard
error of the mean (SEM.)
—Figure S4D, by performing different
normalizing calculations in the
Rescue condition than performed in
other conditions and by omitting
three data points from the Rescue
conditions calculated average
• In Paper 2, Respondent falsified
and/or fabricated the research record in:
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—Figure 1E, by selectively omitting data
points from the analysis
—Figure 2A, by selectively omitting
data points from the analysis
—Figure 2C (left and right), by changing
selected raw measurements by
multiplying with a fixed value to
make the data consistent with data
collected in other experiments
—Figure 5B, by selectively including
and omitting data points from the
analysis
—Figure 5C, by selectively including
and omitting data points from the
analysis
—Figure 7A (right), by reporting that
error bars represented standard
deviation, when they actually
represented standard error of the
mean (SEM.)
ORI found that Respondent engaged
in research misconduct by intentionally,
knowingly, or recklessly falsely
claiming in the methods and results to
have performed validation of deletion/
re-expression of FMNR2 levels in
genetically modified B16 cell lines
when that genetic modification was not
validated for data reported in Figures 7
and 7S of Paper 1.
ORI found that Respondent engaged
in research misconduct by intentionally,
knowingly, or recklessly falsely
reporting a larger number of data points
than actually were collected in fourteen
(14) figures across the two (2) papers
and supplementary materials.
Specifically:
• In Paper 1, Respondent falsified
and/or fabricated the reported data in:
—Figure 2B (top), by reporting ten (10)
cells per condition when nine (9)
Knock Down (KD) and eight (8)
Rescue were included in the analysis
—Figure 2B (middle), by reporting ten
(10) cells per condition when eight (8)
Rescue were included in the analysis
—Figure 3B (top), by reporting twentyfive (25) cells per condition when
nineteen (19) Control, nineteen (19)
KD, and fourteen (14) Rescue were
included in the analysis
—Figure 3B (bottom), by reporting
twenty-five (25) cells per condition
when twenty-four (24) Control and
twenty-three (23) Rescue were
included in the analysis
—Figure 5A, by reporting to have
examined fifty (50) cells per
condition, when only twenty-three
(23), twenty-three (23), and twelve
(12) for the 2mg/mL conditions
(Control, KD, and Rescue,
respectively) and twenty-five (25),
twenty (20), and nine (9) for the 3mg/
mL conditions (Control, KD, and
Rescue, respectively) were recorded
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—Figure 6D, by reporting ten (10) cells
per condition when only eight (8)
Control were recorded
—Figure 7D, by reporting four (4) mice
for each of two (2) independent clones
(8 total) for each condition when only
four (4) Vector+GFP, four (4) WT, and
two (2) B16 conditions were
examined
—Figure S2E (top), by reporting to have
measured two hundred fifty (250)
Focal Adhesions per condition, when
only fifty-six (56) measurements were
recorded for the Leading Edge
Adhesions (LEA) analysis
—Figure S2E (3rd row left and 4th row
left), by reporting twenty-five (25)
cells per condition when only ten (10)
cells were recorded
—Figure S4C, by reporting ten (10) cells
per condition when only five (5) cells
were recorded
—Figure S5B, by reporting ten (10) cells
per condition when only seven (7)
and six (6) cells were recorded for
Control and KD respectively
—Figure S6E, by reporting twenty-five
(25) cells per condition when only
twenty-four (24), eighteen (18), and
sixteen (16) cells were recorded for
Control (48hr), KD (24hr), and KD
(48hr) respectively
• In Paper 2, Respondent falsified
and/or fabricated the reported data in:
—Figure 1E (top), by reporting six (6)
cells per condition when only three
(3) were recorded in Tropomyosin
(Tpm) analysis
—Figure 2C (middle and right), by
reporting twenty (20) cells per
condition when only sixteen (16),
sixteen (16), and five (5) cells were
recorded for Control, KD, and Rescue
respectively
—Figure 3A (right), by reporting the
data from one of four analyses in the
KD condition as the average of five
—Figure 3C (right), by reporting
examination of ten (10) stress fibers
per condition when only three (3),
four (4), and seven (7) cells were
recorded for Control, KD, and Rescue
respectively
—Figure 5B, overstating the number of
adhesions examined
—Figure 5C, overstating the number of
cells examined in all conditions
—Figure 7D (right), by reporting
examination of ten (10) cells per
condition when only five (5), four (4),
and five (5) cells were recorded for
Control, KD, and Rescue respectively
ORI found that Respondent engaged
in research misconduct by intentionally,
knowingly, or recklessly fabricating
results and/or falsely labelling
experimental results that arose from
alternate experimental conditions/
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experiments in seven (7) figures across
the two (2) papers and supplementary
materials. Specifically:
• In Paper 1, Respondent falsified
and/or fabricated the record in:
—Figure 5B (top right), by reporting
results of 8 and 12 um pore migration,
which did not originate from
experimental observations
—Figure 5B (bottom left), by reporting
results for the Rescue condition,
which did not originate from
experimental observations
—Figure 5B (left), by using selected
regions from the same original image
to represent both the control (top) and
rescue conditions (bottom)
—Figure 5C (bottom), by reporting data
derived from 2.5um channels as
originating from 3.5um channels
—Figure 6B (top), by reporting results
for the ‘‘Glass’’ condition (all
treatments) and rescue treatment
(both conditions) that did not
originate from experimental
observations
—Figure 6B (bottom), by reporting
results for the 8um pore condition
that did not originate from
experimental observations
—Figure 6E, by reporting results for the
ATRi and ATMi treatments (Control
and KD conditions) and DMSO
control (Rescue condition) that did
not originate from experimental
observations and reporting results as
originating from DMSO (Control and
KD conditions) controls that had
originated from a different treatment
—Figure 6G, by reporting results for the
‘‘No Drug’’ conditions that did not
originate from experimental
observations
—Figure 6I, by reporting results in all
conditions that originated in part from
the same experimental dataset
reported in Figure 6B (top)
—Figure S4D, by reporting results that
did not originate from experimental
observations for the KD condition
—Figure S6C (right), by shifting selected
data points in the KD condition from
their original time points to different
time points
—Figure S7A, by using bands to
represent FMN2 expression in six
separate conditions, which originated
from different molecular weight
regions in three lanes on the original
Western blot, and by representing
absence of FMN2 expression in two
conditions (CRISPR1 and CRISPR2)
by reporting absence of bands in lanes
in which no protein had been loaded
—Figure S7F (rightmost), by selecting
single data points from different
treatments and reporting them as
means and standard deviations for all
of the treatments
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• In Paper 2, Respondent falsified
and/or fabricated the record in:
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—Figure 2A (top), by reporting results
for the Rescue condition that did not
originate from experimental
observations
—Figure 3C (right), by reporting results
for the Rescue condition that did not
originate from experimental
observations
Dr. Skau entered into a Voluntary
Settlement Agreement and voluntarily
agreed, beginning on January 25, 2018:
(1) To have her research supervised
for a period of three (3) years;
Respondent agreed to ensure that prior
to the submission of an application for
PHS support for a research project on
which Respondent’s participation is
proposed and prior to Respondent’s
participation in any capacity on PHSsupported research, the institution
employing her must submit a plan for
supervision of Respondent’s duties to
ORI for approval; the plan for
supervision must be designed to ensure
the scientific integrity of Respondent’s
research contribution; Respondent
agreed that she will not participate in
any PHS-supported research until a plan
for supervision is submitted and
approved by ORI; Respondent agreed to
maintain responsibility for compliance
with the agreed upon plan for
supervision.
(2) that for a period of three (3) years,
any institution employing her must
submit in conjunction with each
application for PHS funds, or report,
manuscript, or abstract involving PHS
supported research in which
Respondent is involved, a certification
to ORI that the data provided by
Respondent are based on actual
experiments or are otherwise
legitimately derived and that the data,
procedures, and methodology are
accurately reported in the application,
report, manuscript, or abstract;
(3) if no supervisory plan is provided
to ORI, to provide certification to ORI
on annual basis that she has not engaged
in, applied for, or had her name
included on any application, proposal,
or other request for PHS funds without
prior notification to ORI;
(4) to exclude herself voluntarily from
serving in any advisory capacity to PHS
including, but not limited to, service on
any PHS advisory committee, board,
and/or peer review committee, or as a
consultant for a period of three (3) years;
and
(5) to the correction or retraction of:
• Cell 167(6):1571–1585, 2016
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• Proceedings of the National Academy
of Sciences 112(19):E2447–E2456,
2015
Wanda K. Jones,
Interim Director, Office of Research Integrity.
[FR Doc. 2018–03766 Filed 2–22–18; 8:45 am]
BILLING CODE 4150–31–P
DEPARTMENT OF HEALTH AND
HUMAN SERVICES
National Institutes of Health
Center for Scientific Review; Notice of
Closed Meetings
Pursuant to section 10(d) of the
Federal Advisory Committee Act, as
amended, notice is hereby given of the
following meetings.
The meetings will be closed to the
public in accordance with the
provisions set forth in sections
552b(c)(4) and 552b(c)(6), Title 5 U.S.C.,
as amended. The grant applications and
the discussions could disclose
confidential trade secrets or commercial
property such as patentable material,
and personal information concerning
individuals associated with the grant
applications, the disclosure of which
would constitute a clearly unwarranted
invasion of personal privacy.
Name of Committee: Center for Scientific
Review Special Emphasis Panel; Small
Business: Cancer Drug Development and
Therapeutics.
Date: March 19–20, 2018.
Time: 8:00 a.m. to 5:00 p.m.
Agenda: To review and evaluate grant
applications.
Place: Embassy Suites at the Chevy Chase
Pavilion, 4300 Military Road NW,
Washington, DC 20015.
Contact Person: Lilia Topol, Ph.D.,
Scientific Review Officer, Center for
Scientific Review, National Institutes of
Health, 6701 Rockledge Drive, Room 6192,
MSC 7804, Bethesda, MD 20892 301–451–
0131, ltopol@mail.nih.gov.
Name of Committee: Center for Scientific
Review Special Emphasis Panel; Disease
Prevention and Management, Risk Reduction
and Health Behavior Change.
Date: March 19–20, 2018.
Time: 8:00 a.m. to 6:00 p.m.
Agenda: To review and evaluate grant
applications.
Place: Westin Grand, 2350 M Street NW,
Washington, DC 20037.
Contact Person: Michael John McQuestion,
Ph.D., Scientific Review Officer, Center for
Scientific Review, National Institutes of
Health, 6701 Rockledge Drive, Room 3114,
Bethesda, MD 20892, 301–480–1276,
mike.mcquestion@nih.gov.
Name of Committee: Center for Scientific
Review Special Emphasis Panel; PAR17–316:
Biomedical Technology Research Resource
(P41).
Date: March 19, 2018.
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Time: 8:00 a.m. to 6:00 p.m.
Agenda: To review and evaluate grant
applications.
Place: Embassy Suites at the Chevy Chase
Pavilion, 4300 Military Road NW,
Washington, DC 20015.
Contact Person: Mark Caprara, Ph.D.,
Scientific Review Officer, Center for
Scientific Review, National Institutes of
Health, 6701 Rockledge Drive, Room 5156,
MSC 7844, Bethesda, MD 20892, 301–435–
1042, capraramg@mail.nih.gov.
Name of Committee: Center for Scientific
Review Special Emphasis Panel; Topics in
Bacterial Pathogenesis.
Date: March 19, 2018.
Time: 8:00 a.m. to 6:00 p.m.
Agenda: To review and evaluate grant
applications.
Place: Residence Inn Bethesda, 7335
Wisconsin Avenue, Bethesda, MD 20814.
Contact Person: Richard G Kostriken,
Ph.D., Scientific Review Officer, Center for
Scientific Review, National Institutes of
Health, 6701 Rockledge Drive, Room 3192,
MSC 7808, Bethesda, MD 20892, 240–519–
7808, kostrikr@csr.nih.gov.
Name of Committee: Center for Scientific
Review Special Emphasis Panel; Small
Business Hematology.
Date: March 19–20, 2018.
Time: 9:00 a.m. to 5:00 p.m.
Agenda: To review and evaluate grant
applications.
Place: National Institutes of Health, 6701
Rockledge Drive, Bethesda, MD 20892
(Virtual Meeting).
Contact Person: Bukhtiar H. Shah, DVM,
Ph.D., Scientific Review Officer, Center for
Scientific Review, National Institutes of
Health, 6701 Rockledge Drive, Room 4120,
MSC 7802, Bethesda, MD 20892, 301–806–
7314, shahb@csr.nih.gov.
(Catalogue of Federal Domestic Assistance
Program Nos. 93.306, Comparative Medicine;
93.333, Clinical Research, 93.306, 93.333,
93.337, 93.393–93.396, 93.837–93.844,
93.846–93.878, 93.892, 93.893, National
Institutes of Health, HHS)
Dated: February 16, 2018.
Sylvia L. Neal,
Program Analyst, Office of Federal Advisory
Committee Policy.
[FR Doc. 2018–03702 Filed 2–22–18; 8:45 am]
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DEPARTMENT OF HEALTH AND
HUMAN SERVICES
National Institutes of Health
Center for Scientific Review; Notice of
Meeting
Pursuant to section 10(a) of the
Federal Advisory Committee Act, as
amended, notice is hereby given of a
meeting of the Center for Scientific
Review Advisory Council.
The meeting will be open to the
public, with attendance limited to space
available. Individuals who plan to
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]]>Agencies
[Federal Register Volume 83, Number 37 (Friday, February 23, 2018)]
[Notices]
[Pages 8091-8093]
From the Federal Register Online via the Government Publishing Office [www.gpo.gov]
[FR Doc No: 2018-03766]
-----------------------------------------------------------------------
DEPARTMENT OF HEALTH AND HUMAN SERVICES
Office of the Secretary
Findings of Research Misconduct
AGENCY: Office of the Secretary, HHS.
ACTION: Notice.
-----------------------------------------------------------------------
SUMMARY: Findings of research misconduct have been made on the part of
Colleen T. Skau, Ph.D., former postdoctoral fellow in the Cell Biology
and Physiology Center, National Heart, Lung, and Blood Institute
(NHLBI), National Institutes of Health (NIH). Dr. Skau engaged in
research misconduct in research supported by NHLBI, NIH. The
administrative actions, including three (3) years of supervision, were
implemented beginning on January 25, 2018, and are detailed below.
FOR FURTHER INFORMATION CONTACT: Wanda K. Jones, Ph.D., Interim
Director, Office of Research Integrity, 1101 Wootton Parkway, Suite
750, Rockville, MD 20852, (240) 453-8200.
SUPPLEMENTARY INFORMATION:
Colleen T. Skau, Ph.D., National Institutes of Health: Based on
Respondent's admission, an assessment conducted by NIH, and analysis
conducted by ORI in its oversight review, ORI found that Dr. Colleen T.
Skau, former postdoctoral fellow in the Cell Biology and Physiology
Center, NHLBI, NIH, engaged in research misconduct in research
supported by NHLBI, NIH.
ORI found that Respondent engaged in research misconduct by
intentionally, knowingly, or recklessly reporting falsified and/or
fabricated data and/or falsifying and/or fabricating data in the
following two (2) papers:
Cell 167(6):1571-1585, 2016 (hereafter referred to as ``Paper
1'')
Proceedings of the National Academy of Sciences 112(19):E2447-
E2456, 2015 (hereafter referred to as ``Paper 2'')
ORI found that Respondent engaged in research misconduct by
intentional, knowing, or reckless falsification and/or fabrication of
the research record by selectively reporting by inappropriate
inclusion/omission or alteration of data points in ten (10) figures and
falsely reporting the statistical significance based on falsified data
in ten (10) figures across the two (2) papers and supplementary
material. Specifically, ORI found that:
In Paper 1, Respondent falsified and/or fabricated the
research record in:
--Figure 3B, by selectively omitting/including data points in the
Rescue condition
--Figure 5B, by reporting a significant difference between conditions
by performing statistical calculations based on fabricated primary data
--Figure 5C (bottom), by selectively omitting images and conditions
from the analysis
--Figure 6I (bottom left), by reporting data from the same data set as
Figure 6B (top)
--Figure S5B, by reporting statistical significance despite performing
a T test calculation that returned an insignificant p-value
--Figure 7F, by reporting that error bars represented standard
deviation, when they actually represented standard error of the mean
(SEM.)
--Figure S4D, by performing different normalizing calculations in the
Rescue condition than performed in other conditions and by omitting
three data points from the Rescue conditions calculated average
In Paper 2, Respondent falsified and/or fabricated the
research record in:
[[Page 8092]]
--Figure 1E, by selectively omitting data points from the analysis
--Figure 2A, by selectively omitting data points from the analysis
--Figure 2C (left and right), by changing selected raw measurements by
multiplying with a fixed value to make the data consistent with data
collected in other experiments
--Figure 5B, by selectively including and omitting data points from the
analysis
--Figure 5C, by selectively including and omitting data points from the
analysis
--Figure 7A (right), by reporting that error bars represented standard
deviation, when they actually represented standard error of the mean
(SEM.)
ORI found that Respondent engaged in research misconduct by
intentionally, knowingly, or recklessly falsely claiming in the methods
and results to have performed validation of deletion/re-expression of
FMNR2 levels in genetically modified B16 cell lines when that genetic
modification was not validated for data reported in Figures 7 and 7S of
Paper 1.
ORI found that Respondent engaged in research misconduct by
intentionally, knowingly, or recklessly falsely reporting a larger
number of data points than actually were collected in fourteen (14)
figures across the two (2) papers and supplementary materials.
Specifically:
In Paper 1, Respondent falsified and/or fabricated the
reported data in:
--Figure 2B (top), by reporting ten (10) cells per condition when nine
(9) Knock Down (KD) and eight (8) Rescue were included in the analysis
--Figure 2B (middle), by reporting ten (10) cells per condition when
eight (8) Rescue were included in the analysis
--Figure 3B (top), by reporting twenty-five (25) cells per condition
when nineteen (19) Control, nineteen (19) KD, and fourteen (14) Rescue
were included in the analysis
--Figure 3B (bottom), by reporting twenty-five (25) cells per condition
when twenty-four (24) Control and twenty-three (23) Rescue were
included in the analysis
--Figure 5A, by reporting to have examined fifty (50) cells per
condition, when only twenty-three (23), twenty-three (23), and twelve
(12) for the 2mg/mL conditions (Control, KD, and Rescue, respectively)
and twenty-five (25), twenty (20), and nine (9) for the 3mg/mL
conditions (Control, KD, and Rescue, respectively) were recorded
--Figure 6D, by reporting ten (10) cells per condition when only eight
(8) Control were recorded
--Figure 7D, by reporting four (4) mice for each of two (2) independent
clones (8 total) for each condition when only four (4) Vector+GFP, four
(4) WT, and two (2) B16 conditions were examined
--Figure S2E (top), by reporting to have measured two hundred fifty
(250) Focal Adhesions per condition, when only fifty-six (56)
measurements were recorded for the Leading Edge Adhesions (LEA)
analysis
--Figure S2E (3rd row left and 4th row left), by reporting twenty-five
(25) cells per condition when only ten (10) cells were recorded
--Figure S4C, by reporting ten (10) cells per condition when only five
(5) cells were recorded
--Figure S5B, by reporting ten (10) cells per condition when only seven
(7) and six (6) cells were recorded for Control and KD respectively
--Figure S6E, by reporting twenty-five (25) cells per condition when
only twenty-four (24), eighteen (18), and sixteen (16) cells were
recorded for Control (48hr), KD (24hr), and KD (48hr) respectively
In Paper 2, Respondent falsified and/or fabricated the
reported data in:
--Figure 1E (top), by reporting six (6) cells per condition when only
three (3) were recorded in Tropomyosin (Tpm) analysis
--Figure 2C (middle and right), by reporting twenty (20) cells per
condition when only sixteen (16), sixteen (16), and five (5) cells were
recorded for Control, KD, and Rescue respectively
--Figure 3A (right), by reporting the data from one of four analyses in
the KD condition as the average of five
--Figure 3C (right), by reporting examination of ten (10) stress fibers
per condition when only three (3), four (4), and seven (7) cells were
recorded for Control, KD, and Rescue respectively
--Figure 5B, overstating the number of adhesions examined
--Figure 5C, overstating the number of cells examined in all conditions
--Figure 7D (right), by reporting examination of ten (10) cells per
condition when only five (5), four (4), and five (5) cells were
recorded for Control, KD, and Rescue respectively
ORI found that Respondent engaged in research misconduct by
intentionally, knowingly, or recklessly fabricating results and/or
falsely labelling experimental results that arose from alternate
experimental conditions/experiments in seven (7) figures across the two
(2) papers and supplementary materials. Specifically:
In Paper 1, Respondent falsified and/or fabricated the
record in:
--Figure 5B (top right), by reporting results of 8 and 12 um pore
migration, which did not originate from experimental observations
--Figure 5B (bottom left), by reporting results for the Rescue
condition, which did not originate from experimental observations
--Figure 5B (left), by using selected regions from the same original
image to represent both the control (top) and rescue conditions
(bottom)
--Figure 5C (bottom), by reporting data derived from 2.5um channels as
originating from 3.5um channels
--Figure 6B (top), by reporting results for the ``Glass'' condition
(all treatments) and rescue treatment (both conditions) that did not
originate from experimental observations
--Figure 6B (bottom), by reporting results for the 8um pore condition
that did not originate from experimental observations
--Figure 6E, by reporting results for the ATRi and ATMi treatments
(Control and KD conditions) and DMSO control (Rescue condition) that
did not originate from experimental observations and reporting results
as originating from DMSO (Control and KD conditions) controls that had
originated from a different treatment
--Figure 6G, by reporting results for the ``No Drug'' conditions that
did not originate from experimental observations
--Figure 6I, by reporting results in all conditions that originated in
part from the same experimental dataset reported in Figure 6B (top)
--Figure S4D, by reporting results that did not originate from
experimental observations for the KD condition
--Figure S6C (right), by shifting selected data points in the KD
condition from their original time points to different time points
--Figure S7A, by using bands to represent FMN2 expression in six
separate conditions, which originated from different molecular weight
regions in three lanes on the original Western blot, and by
representing absence of FMN2 expression in two conditions (CRISPR1 and
CRISPR2) by reporting absence of bands in lanes in which no protein had
been loaded
--Figure S7F (rightmost), by selecting single data points from
different treatments and reporting them as means and standard
deviations for all of the treatments
[[Page 8093]]
In Paper 2, Respondent falsified and/or fabricated the
record in:
--Figure 2A (top), by reporting results for the Rescue condition that
did not originate from experimental observations
--Figure 3C (right), by reporting results for the Rescue condition that
did not originate from experimental observations
Dr. Skau entered into a Voluntary Settlement Agreement and
voluntarily agreed, beginning on January 25, 2018:
(1) To have her research supervised for a period of three (3)
years; Respondent agreed to ensure that prior to the submission of an
application for PHS support for a research project on which
Respondent's participation is proposed and prior to Respondent's
participation in any capacity on PHS-supported research, the
institution employing her must submit a plan for supervision of
Respondent's duties to ORI for approval; the plan for supervision must
be designed to ensure the scientific integrity of Respondent's research
contribution; Respondent agreed that she will not participate in any
PHS-supported research until a plan for supervision is submitted and
approved by ORI; Respondent agreed to maintain responsibility for
compliance with the agreed upon plan for supervision.
(2) that for a period of three (3) years, any institution employing
her must submit in conjunction with each application for PHS funds, or
report, manuscript, or abstract involving PHS supported research in
which Respondent is involved, a certification to ORI that the data
provided by Respondent are based on actual experiments or are otherwise
legitimately derived and that the data, procedures, and methodology are
accurately reported in the application, report, manuscript, or
abstract;
(3) if no supervisory plan is provided to ORI, to provide
certification to ORI on annual basis that she has not engaged in,
applied for, or had her name included on any application, proposal, or
other request for PHS funds without prior notification to ORI;
(4) to exclude herself voluntarily from serving in any advisory
capacity to PHS including, but not limited to, service on any PHS
advisory committee, board, and/or peer review committee, or as a
consultant for a period of three (3) years; and
(5) to the correction or retraction of:
Cell 167(6):1571-1585, 2016
Proceedings of the National Academy of Sciences 112(19):E2447-
E2456, 2015
Wanda K. Jones,
Interim Director, Office of Research Integrity.
[FR Doc. 2018-03766 Filed 2-22-18; 8:45 am]
BILLING CODE 4150-31-P
